吉西他滨加卡铂与依托泊苷加卡铂治疗晚期食管癌的对照试验  被引量：1

作　　者：董晓鹏[1] 赵小刚[1] 彭传亮[1] 李希波[2] 姜兴涛[1] 王化生[1] 

机构地区：[1]山东大学第二医院胸外科,山东济南250033 [2]山东大学齐鲁医院胸外科,山东济南250012

出　　处：《中国新药与临床杂志》2007年第3期225-228,共4页Chinese Journal of New Drugs and Clinical Remedies

摘　　要：目的:观察吉西他滨+卡铂与依托泊苷+卡铂治疗晚期食管癌的疗效和不良反应。方法:可评价疗效的晚期食管癌病人分为治疗组和对照组。治疗组36例,吉西他滨,d 1,8,1 000 mg·m^(-2)静脉滴注;卡铂,d 1,300 mg·m^(-2);21 d为一个周期。对照组35例,依托泊苷,d 1,2,3,100 mg·m^(-2)静脉滴注;卡铂,d 1,300 mg·m^(-2);21 d为一个周期。比较2组的疗效和不良反应。结果:治疗组和对照组的有效率分别为39％和31％(P=0．511),临床获益率分别为78％和54％(P=0．036),平均肿瘤进展时间分别为(5．8±s 1．7)mo和(5．2±1．8)mo(P=0．871),1年生存率分别为61％和49％(P=0．288)。2组主要不良反应为骨髓抑制和胃肠道反应,治疗有效的病人进食困难和胸痛均缓解。结论:吉西他滨+卡铂治疗晚期食管癌疗效确切,临床获益率高,病人耐受性好,为晚期食管癌的治疗提供了一种新的选择。AIM： To evaluate the difference of efficacies and adverse reactions in advanced esophageal cancer patients treated with gemcitabine plus carboplatin versus etoposide plus carboplatin. METHODS： Eligible patients were randomly assigned to PG （gemcitabine ＋ carboplatin） group （n = 36） and PE （etoposide ＋ carboplatin） group （it = 35）. PG group was treated individually with gemcitabine 1 000 mg·m^-2 iv drip on d 1 and 8, and carboplatin 300 mg·m^-2 iv drip on d 1; PE group individually was treated with etoposide 100 mg·m^-2 iv drip on d 1, 2 and 3, and carboplatin 300 mg·m^-2 iv drip on d 1. Both groups pursued 21 d as a cycle. The response rate, clinical benefit rate, time to progression （TTP）, one-year survival, and side effects were observed and compared. RESULTS： The response rates, clinical benefit rates, mean TTP, one year survival rates were 39 % vs 31% （P=0.511）, 78%vs54% （P=0.036）, （5.8±s 1.7） movs （5.2±1.8） mo （P= 0.871）, and 61% vs 49 % （P = 0.288） in the PG and PE groups, respectively. The major adverse reactions were inhibition Of bone marrow and digestive tract reaction, with no statistical difference between the two groups. Dysphagia and chest pain were decreased in the responding patients. CONCLUSION： Good efficacy and tolerability of the PG regimen offer a new candidate for treating advanced esophageal cancer.

关 键 词：食管肿瘤 药物评价 依托泊苷 吉西他滨 

分 类 号：R735.1[医药卫生—肿瘤] R979.1[医药卫生—临床医学]